Oral composition

Oral composition
US4649044

In an oral composition comprising an amino compound, for example, tranexamic acid and ε-aminocaproic acid, a flavor, a surface-active agent, water, and optionally, a humectant, a binder, and an abrasive, the flavor is at least partially comprised of an aldehyde flavor compatible with the amino compound.

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Patent 4649044
Priority Jun 30 1982
Filed Jun 30 1983
Issued Mar 10 1987
Expiry Mar 10 2004
Inventors Sato, Hiro…
Assg.orig Lion Corpo…
Assg.curr Lion Corpo…
Entity Large
Referenced by 14
References 12
Maint.: EXPIRED

BACKGROUND OF THE IN…
SUMMARY OF THE INVEN…
DETAILED DESCRIPTION…
EXAMPLE 1
EXAMPLE 2
EXAMPLE 3
EXAMPLE 4
EXAMPLE 5
EXAMPLE 6
EXAMPLE 7
EXAMPLE 8
EXAMPLE 9
EXAMPLE 10
EXAMPLE 11
EXAMPLE 12

1. An oral paste composition, comprising:

0.01 to 5% by weight of an antiplasmin agent selected from the group consisting of tranexamic acid, ε-aminocaproic acid and their alkyl ester and aryl ester derivatives,

0.01 to 10% by weight of a flavor mixture,

a surface-active agent and water characterized in that said flavor mixture comprises 0.05 to 90% by weight based on the total weight of the flavor mixture of a compatible aldehyde flavor selected from the group consisting of perillaldehyde, myrtenal, benzaldehyde, anisaldehyde, heliotropin, 3-methylbutanal, 2-methylbutanal, hexanal, 10-undecanal, decanal, citronellal, dodecanal, hydroxycitronellal, α-methylcinnamaldehyde and mixtures thereof wherein said oral paste composition is free of Schiff base discoloration caused by an antiplasmin agent amino group reacting with an aldehyde group of said aldehyde flavors.

2. The composition of claim 1 is a toothpaste.

3. The composition according to claim 1, wherein the aldehyde flavor is selected from the group consisting of perillaldehyde, myrtenal, benzaldehyde, anisaldehyde, and heliotropin.

4. The composition according to claim 1, wherein the aldehyde flavor is selected from the group consisting of 3-methylbutanal, 2-methylbutanal, and hexanal.

5. The composition according to claim 1, wherein the aldehyde flavor is selected from the group consisting of 10-undecenal, decanal, citronellal, dodecanal and hydroxycitronellal.

6. The composition according to claim 1, wherein said flavor is present in an amount of 0.05 to 5% by weight of the composition.

7. The composition according to claim 1, which contains an abrasive.

8. The composition according to claim 1, which further contains a humectant.

9. The composition according to claim 1, which contains a binder.

10. The composition according to claim 1, wherein the aldehyde flavor is α-methylcinnamaldehyde.

BACKGROUND OF THE INVENTION

This invention relates to oral compositions comprising an amino compound, typically, an antiplasmin agent such as tranexamic acid and ε-aminocaproic acid, and a compatible aldehyde flavor.

It is well known in the art to blend an antiplasmin agent such as tranexamic acid and ε-aminocaproic acid in oral compositions. However, the use of an antiplasmin agent introduced a problem of discoloration of oral compositions as disclosed in Japanese Patent Publication No. 55-5484 and U.S. Pat. No. 4,272,513. This discoloration of antiplasmin agent-containing oral compositions is allegedly attributable to reaction of the antiplasmin agent with an aldehyde group in the coexisting flavor. To avoid discoloration, Japanese Patent Publication No. 55-5484 proposes to blend cyclodextrin in antiplasmin agent-containing oral compositions, and U.S. Pat. No. 4,272,513 proposes the use of a flavor substantially free of an aldehyde group.

It was fully anticipated that when antiplasmin agents such as tranexamic acid and ε-aminocaproic acid and other amino compounds were blended in oral compositions, the amino group would react with an aldehyde group in aldehyde type flavors to form a Schiff base which would cause the oral compositions to be colored or discolored. Particularly when either of the amino compound and the aldehyde flavor is an aryl compound, a stable Schiff base would be formed.

Making a number of experiments using various combinations of amino compounds and aldehyde compounds, the inventors have found that while acetaldehyde, cinnamic aldehyde, t-2-hexanal and the like cause amino compound-containing oral compositions to be colored or discolored, there are certain aldehyde flavors which are compatible with amino compounds. That is, amino compound-containing oral compositions are not colored or discolored when particular compatible aldehyde flavors are blended therein. Particularly, although chain hydrocarbon aldehyde flavors having a double bond between the α- and β-positions with respect to the aldehyde group cause coloring or discoloration of amino compound-containing oral compositions, unexpectedly those cyclic aldhyde compounds having the structure ##STR1## wherein the ##STR2## moiety constitutes a segment of the cyclic structure have been found to cause no coloring or discoloration of amino compound-containing oral compositions as long as the compounds are free of a phenolic hydroxyl group. That is, substituted or unsubstituted, phenolic hydroxyl-free cyclic aldehyde compounds having an aldehyde group attached to one of their cyclically concatenating carbon atoms have been found useful as the compatible aldehyde flavors. It has also been found that aliphatic aldehyde compounds having 4 to 7 and 9 to 16 carbon atoms and free of a double bond between the carbon atoms at the α- and β-positions with respect to their aldehyde group are useful as the compatible aldehyde flavors.

SUMMARY OF THE INVENTION

It is, therefore, an object of the present invention to provide an oral composition which comprises an amino compound, but undergoes no coloring or discoloration because the amino acid is combined with a compatible aldehyde flavor.

In an oral composition comprising an amino compound, a flavor, a surface-active agent, water, and optionally, a humectant, a binder, and an abrasive, according to the present invention, the flavor is at least partially comprised of a compatible aldehyde flavor.

In a preferred embodiment of the invention, the compatible aldehyde flavor is selected from substituted and unsubstituted, phenolic hydroxyl-free cyclic aldehyde compounds having an aldehyde group attached to one of their cyclically concatenating carbon atoms. In another preferred embodiment of the invention, the compatible aldehyde flavor is selected from aliphatic aldehyde compounds having 4 to 7 and 9 to 16 carbon atoms and free of a double bond between the carbon atoms at the α- and β-positions with respect to their aldehyde group. Also preferred are aliphatic aldehyde compounds having a double bond between the carbon atoms at the α- and β-positions and a C₁ -C₁2 alkyl group or aralkyl group attached at the α-position with respect to their aldehyde group, the total number of carbon atoms of the compounds being 5 to 16.

According to the present invention, by blending compatible aldehyde flavors in amino compound-containing oral compositions, oral compositions with desired flavor are prevented from being colored or discolored without reducing their effectiveness when the amino compound used is an antiplasmin agent. Particularly, when substituted and unsubstituted, phenolic hydroxyl-free cyclic aldehyde compounds (I) having an aldehyde group attached to one of their cyclically concatenating carbon atoms are used as the compatible aldehyde flavor, a choice of the flavor may be made from an increased variety of flavors so that an oral composition capable of imparting pleasant feel when used in the mouth may be readily obtained in spite of the presence of an amino compound which otherwise causes unpleasant feel. When aliphatic aldehyde compounds (II) having 4 to 7 carbon atoms and free of a double bond between the carbon atoms at the α- and β-positions with respect to their aldehyde group are used as the compatible aldehyde flavor, the resulting oral compositions are improved in flavor emission so that they afford improved initial mouth-feel when applied to the mouth. Furthermore, when aliphatic aldehyde compounds (III) having 9 to 16 carbon atoms and free of a double bond between the carbon atoms at the α- and β-positions with respect to their aldehyde group are used as the compatible flavor, the resulting oral compositions are improved in lingering flavor so that they leave an improved aftertaste in the mouth. Aliphatic aldehyde compounds (IV) possessing 5 to 16 carbon atoms in total and having a double bond between the carbon atoms at the α- and β-positions and a C₁ -C₁2 alkyl group or aralkyl group attached at the α-position with respect to their aldehyde group are also effective in improving flavor. While it has been a problem that oral compositions having, for example, tranexamic acid blended taste bitter and leave an unpleasant aftertaste in the mouth, the present invention has succeeded in improving the aftertaste of such compositions.

The above and other objects, features and advantages of the present invention will become more apparent and understandable from the following descriptions.

DETAILED DESCRIPTION OF THE INVENTION

The feature of the present invention is to add to an oral composition containing an amino compound an aldehyde flavor which is compatible with the amino compound and does not cause coloring or discoloration of the composition.

The compatible aldehyde flavor may be selected from the aldehyde compounds which are compatible with amino compounds. More particularly, it may be a substituted or unsubstituted, phenolic hydroxyl-free cyclic aldehyde compound (I) having an aldehyde group attached to one of its cyclically concatenating carbon atoms; an aliphatic aldehyde compound (II) having 4 to 7 carbon atoms and free of a double bond between the carbon atoms at the α- and β-positions with respect to its aldehyde group; an aliphatic aldehyde compound (III) having 9 to 16 carbon atoms and free of a double bond between the carbon atoms at the α- and β-positions with respect to its aldehyde group; and an aliphatic aldehyde compound (IV) having a double bond between the carbon atoms at the α- and β-positions and a C₁ -C₁2 alkyl group or aralkyl group attached at the α-position with respect to its aldehyde group, the total number of carbon atoms of the compound being 5 to 16.

The cyclic aldehyde flavors (I) may be either cycloaliphatic or aromatic compounds as long as they have no phenolic hydroxyl group attached to any member of their cyclic structure. Further, the aliphatic compounds may or may not have an unsaturated bond in their cyclic structure. The cyclic aldehyde flavors (I) may also be either unsubstituted cyclic compounds having no substituent other than the aldehyde group and hydrogen atoms attached to the members of their cyclic structure or substituted cyclic compounds having one or more substituents attached to any member of their cyclic structure in addition to the aldehyde group and hydrogen atoms, the substituents being an alkyl group, alkenyl group, alkoxy group and oxygen atom, for example. In the event of cyclic compounds having an unsaturated bond in their cyclic structure, those compounds having an aldehyde group attached to one of the carbon atoms of the unsaturated bond may be used.

Preferred examples of the cyclic aldehyde flavors (I) include benzaldehyde, 2,4-dimethylbenzaldehyde, cuminaldehyde, p-t-butylbenzaldehyde, heliotropin, anisaldehyde, acetylvanillin, 2,4-di-t-butyl-5-methoxybenzaldehyde, 3-t-butyl-4-methoxybenzaldehyde, p-dimethylresorcylic aldehyde, diisopropyldimethylbenzaldehyde, diisopropylmethylbenzaldehyde, p-ethoxybenzaldehyde, tolylaldehyde, ethylbenzaldehyde, 3-methoxy-4-ethoxybenzaldehyde, o-methoxybenzaldehyde, 4-methoxy-3-methylbenzaldehyde, veratraldehyde, myrtenal, dihydromyrtenal, perillaldehyde, 5-(3-buten-2-yl)-3-cyclohexenecarboxylaldehyde, 5-(3-buten-2-yl)-1-methyl-3-cyclohexenecarboxyaldehyde, decahydro-β-naphthaldehyde, dicyclopentadienaldehyde, 6-methoxydicyclopentadienaldehyde, dihydrocyclocitral, α-cyclocitral, β-cyclocitral, isocyclocitral, dehydro-β-cyclocitral, 2,4-dimethylcyclohex-3-enaldehyde, 3,4-dimethylcyclohexen-5-ylcarboxyaldehyde, 4-(4-methyl-4-hydroxyamyl)-3-cyclohexenecarboxyaldehyde, 1-methyl-4-(4-methyl-3-pentenyl)-3-cyclohexenecarboxyaldehyde, 4-(4-methyl-3-penten-1-yl)-3-cyclohexane-1-carboxyaldehyde, 4-methylsafranal, phellandral, Δ²,3 -2,5,5,9-tetramethyldecalyl-1-ethanal, Δ¹,2 -2,5,5,9-tetramethyldecalyl-1-ethanal, tetrahydro-p-tolylaldehyde, cyclohexanecarboxyaldehyde, etc. Particularly preferred are perillaldehyde, myrtenal, benzaldehyde, anisaldehyde, and heliotropin. Since such cyclic aldehyde flavors can be used as the compatible flavor in oral compositions containing amino compounds according to the present invention, there are obtained oral compositions presenting more pleasant feel.

The aliphatic aldehyde flavors (II) having 4 to 7 carbon atoms may be either saturated or unsaturated chain compounds which may be of either linear or branched chain and may partially form a cyclic structure. They may be either unsubstituted compounds or substituted compounds having a hydroxyl group, alkoxy group or other groups attached to their skeleton as long as they have 4 to 7 carbon atoms in total and are free of a double bond between the carbon atoms at the α- and β-positions with respect to their aldehyde group.

Examples of the aliphatic aldehyde flavors (II) having 4 to 7 carbon atoms include 3-methylbutanal, 2-methylbutanal, hexanal, heptanal, cis-4-heptenal, trans-4-heptenal, pentanal, 2-ethylbutanal, γ-hydroxycaproic aldehyde, δ-hydroxyvaleric aldehyde, 3-methylthiopropanal, 2-methyl-propanal, etc. Particularly preferred are 3-methylbutanal, 2-methylbutanal, and hexanal. By using these aliphatic aldehyde flavors having 4 to 7 carbon atoms, amino compound-containing oral compositions display improved flavor emission so that they afford improved initial flavor and pleasant feel in the mouth.

The aliphatic aldehyde flavors (III) having 9 to 16 carbon atoms may also be either saturated or unsaturated chain compounds which may be of either linear or branched chain and may partially form a cyclic structure. They may be either unsubstituted compounds or substituted compounds having a hydroxyl group, alkoxy group or other groups attached to their skeleton as long as they have 9 to 16 carbon atoms in total and are free of a double bond between the carbon atoms at the α- and β-positions with respect to their aldehyde group.

Examples of the aliphatic aldehyde flavors (III) having 9 to 16 carbon atoms include nonanal, decanal, undecanal, dodecanal, tridecanal, tetradecanal, pentadecanal, hexadecanal, 2,6-dimethyl-5-heptenal, 10-undecenal, 2-methylnonanal, 2-methylundecanal, 2-methyldecanal, 2,6-dimethyloctanal, cis-6-nonenal, citronellal, dihydrocitronellal, hydroxycitronellal, methoxycitronellal, isocitronellal, β-hydroxypelargonic aldehyde, 3-methylnonanal, 2-methyloctanal, 3-methylcitronellal, 3,5,5-trimethylhexanal, n-octyloxyacetaldehyde, decyloxyacetaldehyde, 10,11-dimethyldodecanal, amylheptylacetaldehyde, citronellyloxyacetaldehyde, geranylisobutyraldehyde, geranoxyacetaldehyde, hydroxycitronellyl ethyl carbonate, hexahydrofarnesol, 9-undecenal, cis-8-undecen-1-al, cis-4-undecen-1-al, 3-methyldodecanal, α-methyldodecanal, 3-methyltridecanal, 2,6,10-trimethyl-9-undecen-1-al, 2,6,10-trimethylundecanal, decahydro-β-naphthylacetaldehyde, α-ethyl-2,2,6-trimethylcyclohexanebutyric aldehyde, β-(4-methylcyclohexyl)-butyraldehyde, 2-methyl-4-(2,6,6-trimethyl-1-cyclohexenyl)-3-buten-1-al, 2-methyl-4-(2,6,6-trimethyl-2-cyclohexenyl)-3-buten-1-al, β-(4-methyl-3-cyclohexenyl)-butyraldehyde, p-t-amylphenoxyacetaldehyde, m-chlorohydrocinnamic aldehyde, cyclamen aldehyde, p-isobutylhydrocinnamic aldehyde, α-amylhydrocinnamic aldehyde, p-t-butyl-α-methylhydrocinnamic aldehyde, p-ethyl-α,α-dimetylhydrocinnamic aldehyde, α-ethylhydrocinnamic aldehyde, β-benzoxypropionic aldehyde, p-methoxyphenoxyacetaldehyde, α-methylhydrocinnamic aldehyde, p-methylhydrocinnamic aldehyde, 2-methyl-4-phenylbutyraldehyde, 3-methyl-4-phenylvaleric aldehyde, 2-methyl-3-p-tolylpropionaldehyde, α-methyl-3,4-methylenedioxyhydrocinnamic aldehyde, phenetoxyacetaldehyde, 4-phenylbutanal, hydrocinnamic aldehyde, p-isopropylbenzylbutyraldehyde, p-n-propylmethylhydrocinnamic aldehyde, 3-(1-isopropylphenyl)-propionic aldehyde, etc. Particularly preferred are 10-undecenal, decanal, citronellal, and hydroxycitronellal.

The use of these aliphatic aldehyde flavors having 9 to 16 carbon atoms provides a substantial improvement in the lingering flavor of oral compositions containing amino compounds, and particularly, when tranexamic acid is blended in oral compositions, the concomitant bitterness and unpleasant aftertaste are substantially eliminated.

α-methylcinnamaldehyde is a typical example of the aliphatic aldehyde compounds (IV) possessing 5 to 16 carbon atoms in total and having a double bond between the carbon atoms at the α- and β-positions and a C₁ -C₁2 alkyl group or aralkyl group attached at the α-position with respect to their aldehyde group.

In the practice of the invention, the above-mentioned compatible aldehyde flavors may be used alone or in admixture of two or more while combinations of the cyclic aldehyde flavors with the aliphatic aldehyde flavors having 4-7 and 9-16 carbon atoms are preferred because of enhanced pleasant feel. It is to be noted that the compatible aldehyde flavors are usually available as being synthesized or isolated from essential oils. Such synthesized or isolated aldehyde flavors may be blended in oral compositions although the compatible aldehyde flavor may be blended in the form of an essential oil containing it without isolation.

In addition to the compatible aldehyde flavors, the oral compositions of the invention may further contain one or more other flavors, for example, isolated or synthetic flavors such as l-menthol, carvone, anethole, eugenol, cineole, vanillin, zingerone, isoeugenol, guaiacol, creosol, thymol, methyl salicylate, isobutyl salicylate, amyl salicylate, methyl-para-cresol, linalool, etc., and essential oils such as spearmint oil, peppermint oil, anise oil, sage oil, rosemary oil, eucalyptus oil, wintergreen oil, sassafras oil, clove oil, majoram oil, orange oil, strawberry flavor, etc. The presence of the compatible aldehyde flavors allows incompatible aldehyde flavors such as cinnamic aldehyde and salycylic aldehyde to be blended in amino compoundcontaining oral compositions in such an amount that they may not be discolored at all.

In the practice of the invention, a flavor mixture may be previously prepared from two or more of the compatible aldehyde flavors or one or more of the compatible aldehyde flavors and one or more other flavors before it is subsequently blended in oral compositions.

The amount of the compatible aldehyde flavors blended is not particularly limited although it may preferably be blended in an amount of at least 0.01% by weight, especially 0.05 to 90% by weight based on the flavor mixture or the total weight of flavors. In turn, the flavor mixture comprised of the compatible aldehyde flavor may preferably be blended in oral compositions in an amount of 0.01 to 10% by weight, especially 0.05 to 5% by weight of the composition.

According to the present invention, the compatible aldehyde flavors are blended in oral compositions containing amino compounds as described above. As the amino compounds, use may be made of one or more of amino acids, peptides, proteins (including enzymes), amino acid type bactericides, amino acid type surfactants, and antiplasmin agents. Examples of the amino acids include glycine, alanine, β-alanine, glutamic acid, cystine, serine, phenylalanine, etc. Examples of the peptides include caropeptide, glutathione, glycylglycine, aspartylphenylalanyl methyl ester, and peptide type anti-allergy agents. Examples of proteins include gelatin, peptone, albumin, casein, etc. and examples of the enzymes include dextranase, amylase, protease, mutanase, lysozyme and lytic enzyme, etc. Further, examples of the antiplasmin agents include tranexamic acid, ε-aminocaproic acid and their derivatives, for example, alkyl ester derivatives such as hexyl tranexamate, phenyl tranexamate, hexyl ε-aminocaproate, and heptyl ε-aminocaproate, and aryl ester derivatives. Since the use of the compatible aldehyde flavors in combination with the antiplasmin agent prevents the resulting oral compositions from being colored or discolored and improves the unpleasant feel concomitant with the antiplasmin agent, the present invention is particularly advantageously applied to oral compositions containing antiplasmin agents.

The amount of the amino compounds blended varies with their type although they are blended in oral compositions generally in an mount of 0.001 to 10% by weight of the composition. In the case of antiplasmin agents, they are preferably blended in an amount of 0.01 to 5% by weight of the composition.

The oral compositions according to the present invention encompass a variety of oral compositions, for example, dentifrices such as toothpaste, tooth powder and liquid dentifrice, liquid oral refreshers such as mouthwash, solid oral refreshers such as troches, chewing gums, oral pastes and the like. In addition to the above-mentioned ingredients, any suitable ingredients may be selected and blended in the oral compositions of the present invention depending on their type.

More specifically, for dentifrices, abrasives may be blended in an amount of 20-90% by weight (for toothpastes, 20-60% by weight), including dicalcium phosphate dihydrate and anhydride, calcium primary phosphate, calcium tertiary phosphate, calcium carbonate, calcium pyrophosphate, aluminum hydroxide, alumina, silicic anhydride, silica, silica gel, aluminosilicate, aluminum silicate, insoluble sodium metaphosphate, magnesium tertiary phosphate, magnesium carbonate, calcium sulfate, polymethyl methacrylate, bentonite, zirconium silicate, etc. and mixtures thereof.

For pasty compositions, for example, toothpastes, a binder may be blended in an amount of 0.3 to 5% by weight, including synthetic binders such as carrageenan, cellulose derivatives such as sodium carboxymethylcellulose, methyl cellulose, hydroxyethylcellulose, sodium carboxymethylhydroxyethylcellulose, alkali metal alginates such as sodium alginate, propylene glycol alginate, gums such as xanthane gum, tragacanth gum, karaya gum, gum arabic, etc. polyvinyl alcohol, sodium polyacrylate, carboxyvinyl polymer, polyvinyl pyrrolidone, etc. and inorganic binders such as silica gel, aluminum silicate gel, veegum, laponite, etc. and mixtures thereof.

In preparing pasty and liquid oral compositions such as toothpastes and mouthwashes, a humectant may be blended in an amount of 10 to 70% by weight, including sorbitol, glycerine, ethylene glycol, propylene glycol, 1,3-butylene glycol, polyethylene glycol, polypropylene glycol, xylitol, maltitol, lactitol, etc. and mixtures thereof.

Also included are anionic surfactants such as watersoluble salts of higher alkyl sulfates (e.g., sodium lauryl sulfate), sodium salts of higher fatty acids, water-soluble salts of sulfonated monoglycerides of higher fatty acids having 10 to 18 carbon atoms in the fatty acid group (e.g., sodium lauryl monoglyceride sulfonate and sodium coconut monoglyceride sulfonate), higher fatty acid sodium monoglyceride monosulfates, olefin sulfonates, paraffin sulfonates; nonionic surfactants such as fatty acid mono- and di-ethanol amides (e.g., lauroyl mono- and di-ethanol amides), stearyl monoglyceride, sucrose fatty acid esters having 12 to 18 carbon atoms in the fatty acid group (e.g., sucrose monolaurate and dilaurate), lactose fatty acid esters, lactitol fatty acid esters, maltitol fatty acid esters, stearic acid monoglyceride, polyoxyethylene sorbitan monolaurate, polyoxyethylene-hardened castor oil, condensates of sorbitan monostearate with approximately 60 moles of ethylene glycol, condensates of ethylene oxide with propylene oxide and their derivatives (e.g., polyoxyethylene polyoxypropylene monolauryl ester), etc.; and amphoteric surfactants such as those of betaine type, etc., alone or in admixture of two or more in an amount of 0 to 10% by weight, preferably 0.1 to 5% by weight.

Also included in the oral compositions according to the present invention are a sweetener such as sodium saccharin, stevioside, neohesperidin dihydrocalcone, glycyrrhizin, perillartine, thaumatin, fractose, sodium cyclaminate, etc. in an amount of 0 to 1% by weight, preferably 0.01 to 0.5% by weight; an antiseptic agent such as p-hydroxymethylbenzoic acid, p-hydroxyethylbenzoic acid, p-hydroxypropylbenzoic acid, p-hydroxybutylbenzoic acid, sodium benzoate, lower fatty acid monoglycerides, etc.; titanium dioxide, ethanol, liquid paraffin, coloring matter, and other additives. For example, toothpastes may be prepared by kneading the desired ingredients selected from the foregoing ingredients with a proper amount of water.

Other types of oral compositions may also be prepared in a conventional manner by selecting commonly used ingredients for the respective types.

In this case, the pH of pasty and liquid oral compositions generally falls in the range of 5 to 10 although not particularly limited thereto.

In the practice of the invention, also blended are one or more active ingredients, for example, alkali metal monofluorophosphates such as sodium monofluorophosphate and potassium monofluorophosphate, fluorides such as sodium fluoride and stannous fluoride, chlorohexidine salts, aluminum chlorohydroxylallantoin, dihydrocholesterol, glycyrrhizin salts, glycyrrhetinic acid, glycerophosphate, chlorophyll, sodium chloride, caropeptide, quaternary ammonium compounds, water-soluble inorganic phosphoric acid compounds, etc.

According to the present invention, by blending a compatible aldehyde flavor in an oral composition containing an amino compound, the resulting oral composition is stable are resistant to discoloration. The blending of the aldehyde flavors imparts to oral compositions pleasant flavor, fine taste and good body as being felt brilliant, sweet or mild. By using the aldehyde flavors alone or in admixture with other flavors, oral compositions containing antiplasmin agents which are previously believed to be unfavorable in flavor and taste can be provided with pleasant feel.

Examples of the present invention are set forth below by way of illustration and not by way of limitation. All percents are by weight.

EXAMPLE 1

Three types of mouthwashes were prepared according to the following formulation: mouthwashes A having aldehyde flavors shown in Table 1 and tranexamic acid, mouthwashes B having the same formulation as mouthwashes A except that tranexamic acid was excluded, and mouthwashes C having the same formulation as mouthwashes A except that the aldehyde flavor was excluded. The tone of the mouthwashes was visually observed both immediately after preparation and after aging at 50°C for two days, to evaluate their stability. The results are shown in Table 1.

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Mouthwash

Formulation (% by weight)

A B C

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Tranexamic acid 0.2 -- 0.2

Carvone 0.2 0.2 0.2

l-Menthol 0.2 0.2 0.2

Aldehyde flavor 0.2 0.2 --

Ethanol 12.0 12.0 12.0

Polyoxyethylene-hardened

4.5 4.5 4.5

castor oil

Glycerin 10.0 10.0 10.0

Sodium saccharin 0.5 0.5 0.5

Water Balance Balance Balance

100.0 100.0 100.0

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TABLE 1

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Mouthwash

Aldehyde A B C

flavor Fresh Aged Fresh Aged Fresh Aged

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3-Methyl-

-- -- -- -- -- --

butanal

2-Methyl-

-- -- -- -- -- --

butanal

Hexanal -- -- -- -- -- --

Decanal -- -- -- -- -- --

Dodecanal

-- -- -- -- -- --

10-Undecenal

-- -- -- -- -- --

Citronellal

-- -- -- -- -- --

Hydroxy- -- -- -- -- -- --

citronellal

Perillalde-

-- -- -- -- -- --

hyde

Myrtenal -- -- -- -- -- --

Benzaldehyde

-- -- -- -- -- --

Anisaldehyde

-- -- -- -- -- --

Heliotropin

-- -- -- -- -- --

α-Methyl-

-- -- -- -- -- --

cinnamalde-

hyde

Acetaldehyde

-- P -- -- -- --

Cinnamic -- Y -- -- -- --

aldehyde

Propanal -- Y -- -- -- --

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Note: -- colorless; P pink; Y yellow.

As apparent from Table 1, the mouthwashes having acetaldehyde, cinnamic aldehyde and propanal blended with tranexamic acid were discolored whereas the mouthwashes having the remaining aldehyde flavors blended with tranexamic acid were not discolored at all.

For those mouthwashes which contained both the aldehyde flavors and tranexamic acid and had not been discolored, the tranexamic acid was analyzed after two-days aging at 50°C to find that its content was unchanged, that is, the mouthwashes retained their efficacy.

When 0.76% of sodium monofluorophosphate was further added to the mouthwashes containing both tranexamic acid and the compatible aldehyde flavors, no change of color was observed.

Similar results were obtained when ε-aminocaproic acid was used instead of tranexamic acid.

EXAMPLE 2

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Toothpaste

______________________________________

Dicalcium phosphate 50%

Silicic anhydride 2

Propylene glycol 3

Sorbitol 10

Glycerin 10

Sodium saccharin 0.1

Higher C₁0 -C₁6 alcohol lauryl sulfate*

1.5

Sodium carboxymethyl cellulose

0.5

Carrageenan 0.5

Tranexamic acid 0.1

Flavor mixture No. 1 1.0

Water Balance

100.0%

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*C₁0 0-2%, C₁2 50-80%, C₁4 10-30%, C₁6 0-10%

Flavor mixture No. 1 used in this example has the following composition:

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Carvone 80%

l-Menthol 14.38

Benzaldehyde 0.01

Perillaldehyde 0.01

Coriander oil 0.1

Orange oil 0.5

Ethanol 5

100.0%

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EXAMPLE 3

______________________________________

Toothpaste

______________________________________

Dicalcium phosphate 50%

Glycerin 20

Sodium saccharin 0.1

Perillartine 0.01

Sodium lauryl sulfate

2.0

Sodium carboxymethyl cellulose

1.0

Tranexamic acid 0.03

Sodium monofluorophosphate

0.76

Flavor mixture No. 2 1.5

Water Balance

100.0%

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Flavor mixture No. 2 used in this example has the following composition:

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Carvone 40%

l-Menthol 40

Anethole 8.6

Benzaldehyde 0.05

Anisaldehyde 0.03

Decanal 0.02

Myrtenal 1.0

Methyl salicylate

10.0

Sage oil 0.1

Orange oil 0.1

Cardamon oil 0.1

100.0%

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EXAMPLE 4

______________________________________

Toothpaste

______________________________________

Aluminum hydroxide 50%

Propylene glycol 2

Sorbitol 20

Sodium saccharin 0.05

Sodium lauryl sulfate

1.2

Sodium carboxymethyl cellulose

0.8

Carrageenan 0.3

Tranexamic acid 0.05

ε-Aminocaproic acid

0.1

Flavor mixture No. 3 0.8

Water Balance

100.0%

______________________________________

Flavor mixture No. 3 used in this example has the following composition:

______________________________________

Carvone 20%

l-Menthol 20

Peppermint oil 9

Spearmint oil 20

Anethole 5

Heliotropin 0.2

Anisaldehyde 0.3

Decanal 0.5

Eugenol 1

Cineole 5

Linalool 5

Ethanol 14

100.0%

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EXAMPLE 5

______________________________________

Toothpaste

______________________________________

Aluminum hydroxide 40%

Silicic anhydride 3

Sorbitol 5

Glycerin 20

Sodium saccharin 0.2

Higher C₁0 -C₁6 alcohol lauryl sulfates*

0.5

Lauroyl diethanol amide

1.5

Carrageenan 0.8

Sodium alginate 0.5

ε-Aminocaproic acid

1.0

Sodium monofluorophosphate

0.76

Dextranase (10⁶ U/g)

0.2

Gelatin 0.5

Flavor mixture No. 4 1.3

Water Balance

100.0%

______________________________________

*C₁0 0-2%, C₁2 50-80%, C₁4 10-30%, C₁6 0-10%

Flavor mixture No. 4 used in this example has the following composition:

______________________________________

Carvone 10%

l-Menthol 40

Peppermint oil 10

Spearmint oil 33.4

Benzaldehyde 3

Hexanal 1

α-methylcinnamaldehyde

Thymol 0.1

Sage oil 0.5%

Cardamon oil 1

100.0%

______________________________________

EXAMPLE 6

______________________________________

Toothpaste

______________________________________

Dicalcium phosphate 20%

Aluminum hydroxide 30

Propylene glycol 1

Sorbitol 8

Glycerin 15

Stevioside 0.1

Sodium lauryl sulfate

1.0

Carrageenan 1.0

Tranexamic acid 0.5

Chlorohexidine hydrochloride

0.1

Flavor mixture No. 5 1.0

Water Balance

100.0%

______________________________________

Flavor mixture No. 5 used in this example has the following composition:

______________________________________

Carvone 20%

l-Menthol 66

2-Methylbutanal 2

3-Methylbutanal 33

Citronellal 2

Perillaldehyde 2

10-Undecenal 1

Linalool 0.5

Orange oil 0.5%

Ethanol 3

100.0%

______________________________________

EXAMPLE 7

______________________________________

Toothpaste

______________________________________

Silicic anhydride 20%

Sorbitol 20

Glycerin 40

Sodium saccharin 0.1

Aspartylphenylallanine methyl ester

0.01

Sodium lauryl sulfate 3.0

Sodium alginate 1.0

ε-Aminocaproic acid

0.05

Flavor mixture No. 6 2.0

Water Balance

100.0%

______________________________________

Flavor mixture No. 6 used in this example has the following composition:

______________________________________

Carvone 30%

l-Menthol 20

Peppermint oil 20

Benzaldehyde 8

Decanal 10

3-Methylbutanal 10

Hydroxycitronellal

Myrtenal 1

100.0%

______________________________________

EXAMPLE 8

______________________________________

Liquid dentifrice

______________________________________

Calcium carbonate 80%

Glycerin 10

Stevioside 0.01

Perillartine 0.1

Higher C₁0 -C₁6 alcohol lauryl sulfates*

0.5

Tranexamic acid 0.1

Aluminum chlorohydroxyallantoinate

0.1

Dipotassium glycyrrhizin

0.1

Flavor mixture No. 7 0.5

Water Balance

100.0%

______________________________________

*C₁0 0-2%, C₁2 50-80%, C₁4 10-30%, C₁6 0-10%

Flavor mixture No. 7 used in this example has the following composition:

______________________________________

Carvone 10%

l-Menthol 10

Anisaldehyde 20

Decanal 20

2-Methylbutanal 20

Perilla oil 20

100.0%

______________________________________

EXAMPLE 9

______________________________________

Toothpaste

______________________________________

Calcium carbonate 40%

Silicic anhydride 3

Propylene glycol 3

Sorbitol 10

Glycerin 15

Stevioside 0.1%

Sodium lauryl sulfate

1.5

Sodium carboxymethyl cellulose

1.0

Tranexamic acid 2.0

Sodium chloride 10.0

Flavor mixture No. 8 1.2

Water Balance

100.0

______________________________________

Flavor mixture No. 8 used in this example has the following composition:

______________________________________

Carvone 80%

l-Menthol 8

Benzaldehyde 5

Anisaldehyde 1

Decanal 1

3-Methylbutanal 1

Citronellal 1

Perillaldehyde 1

Eugenol 1

Orange oil 2

100.0%

______________________________________

EXAMPLE 10

______________________________________

Liquid dentifrice

______________________________________

Glycerin 35%

Propylene glycol 5.0

Sodium polyacrylate

3.0

Sodium lauryl sulfate

1.0

Sodium saccharin 0.2

Ethanol 3.0

Tranexamic acid 3.0

Flavor mixture No. 9

2.0

Water Balance

100.0%

______________________________________

Flavor mixture No. 9 used in this example has the following composition:

______________________________________

Carvone 15%

l-Menthol 40

Peppermint oil 20

Spearmint oil 15

Benzaldehyde 5

Cineole 5

100.0%

______________________________________

EXAMPLE 11

______________________________________

Mouthwash

______________________________________

Ethanol (90%) 20%

Sodium saccharin 0.3

Polyoxyethylene-hardened castor oil

0.5

ε-Aminocaproic acid

0.05

Flavor mixture No. 10 3.0

Water Balance

100.0%

______________________________________

Flavor mixture No. 10 used in this example has the following composition:

______________________________________

Carvone 20%

l-Menthol 50

Anethole 10

Eugenol 5

Linalool 2

Myrtenal 2

Perillaldehyde 3

Cineole 8

100.0%

______________________________________

EXAMPLE 12

______________________________________

Oral paste

______________________________________

Liquid paraffin 26%

Sorbitol 5

Glycerin 15

Cetanol 4

Paraffin wax 6

Microcrystalline wax 10

Polyoxyethylene sorbitan monooleate

Tranexamic acid 0.1

Flavor mixture No. 11 1.0

Water Balance

100.0%

______________________________________

Flavor mixture No. 11 used in this example has the following composition:

______________________________________

Carvone 10%

l-Menthol 40

Anethole 5

Peppermint oil 15

Spearmint oil 15

Eugenol 5

Thymol 5

Perillaldehyde 2

Hexanal 2

Citronellal 1

100.0%

______________________________________

The oral compositions of Examples 2-12 were all resistant to coloring and discoloration and gave pleasant feel when applied to the mouth.

INVENTORS:

Sato, Hiroshi, Ishii, Kazuo, Gomi, Tetsuo, Suganuma, Nobuo

THIS PATENT IS REFERENCED BY THESE PATENTS:

Patent	Priority	Assignee	Title
11666532,	Jan 19 2018	Hyloris Developments SA	Tranexamic acid oral solution
4774076,	Jun 30 1982	Lion Corporation	Oral composition
5015464,	Mar 26 1986	Access Business Group International LLC	Antiplaque chewing gum
5098891,	Mar 17 1988	Institut Straumann AG	Protein composition inducing a binding between parts of mineralized tissue
5472684,	Jun 02 1993	Colgate-Palmolive Company	Oral compositions for plaque and gingivitis
5534243,	Sep 26 1994	The Procter & Gamble Company; Procter & Gamble Company, The	Aqueous oral compositions
5681549,	Jun 10 1994	The Procter & Gamble Company	Mouthrinse compositions
5686063,	Jun 10 1994	The Procter & Gamble Company	Mouthrinse compositions
6835709,	Jul 09 1999	Shiseido Co., Ltd.	Stimulative agent and stimulative perfume composition
7316833,	Jun 24 1993	Exopack, LLC	Multi-layer thermoplastic films and packages made therefrom
7741267,	Aug 04 2004	Firmenich S.A.	Citronella and floral perfuming ingredient
8765155,	Aug 30 2007	Colgate-Palmolive Company	Oral care strip or tape and methods of use and manufacture thereof
8962057,	Apr 29 2009	The Procter & Gamble Company	Methods for improving taste and oral care compositions with improved taste
9724541,	Apr 06 2009	Lisa Marie, Kao	Dental cleaning and polishing composition comprising diamond particles

THIS PATENT REFERENCES THESE PATENTS:

Patent	Priority	Assignee	Title
3497590,
3651206,
3679792,
3749766,
3920840,
4048299,	Jan 10 1969	William Wrigley, Jr. Co.	Anticaries confectionaries and oral health products
4465662,	Apr 02 1981	Lion Corporation	Oral compositions of tranexamic acid and carvone
GB2068229,
GB2073019,
JP4939818,
JP7439818,
JP81142205,

ASSIGNMENT RECORDS Assignment records on the USPTO

/////

Executed on	Assignor	Assignee	Conveyance	Frame	Reel	Doc
Jun 17 1983	GOMI, TETSUO	Lion Corporation	ASSIGNMENT OF ASSIGNORS INTEREST	004149	0852	pdf
Jun 17 1983	SUGANUMA, NOBUO	Lion Corporation	ASSIGNMENT OF ASSIGNORS INTEREST	004149	0852	pdf
Jun 17 1983	ISHII, KAZUO	Lion Corporation	ASSIGNMENT OF ASSIGNORS INTEREST	004149	0852	pdf
Jun 17 1983	SATO, HIROSHI	Lion Corporation	ASSIGNMENT OF ASSIGNORS INTEREST	004149	0852	pdf
Jun 30 1983		Lion Corporation	(assignment on the face of the patent)

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Jun 23 1993	ASPN: Payor Number Assigned.
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Mar 12 1995	EXP: Patent Expired for Failure to Pay Maintenance Fees.

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